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早期类风湿关节炎患者滑膜组织中动态T细胞受体克隆型变化:环孢素A(新山地明)治疗的影响

Dynamic T cell receptor clonotype changes in synovial tissue of patients with early rheumatoid arthritis: effects of treatment with cyclosporin A (Neoral).

作者信息

VanderBorght Ann, De Keyser Filip, Geusens Piet, De Backer Marc, Malaise Michel, Baeten Dominique, Van den Bosch Filip, Veys Eric M, Raus Jef, Stinissen Piet

机构信息

Biomedisch Onderzoeksinstituut DWI, Limburgs Universitair Centrum, Diepenbeek, Belgium.

出版信息

J Rheumatol. 2002 Mar;29(3):416-26.

Abstract

OBJECTIVE

To study T cell receptor (TCR) repertoire changes in synovial membrane over a 16 week period in patients with early rheumatoid arthritis (RA); and to study the influence of cyclosporin A (CSA) on TCR repertoire in a subgroup of these patients.

METHODS

Synovial tissue biopsies and paired blood samples were obtained from 12 patients with early RA at 2 time points. Seven patients were treated with CSA (Neoral-Sandimmun, 3 mg/kg/day) and 5 patients with placebo for 16 weeks. TCR V gene repertoires were analyzed by semiquantitative PCR-ELISA. CDR3 spectratyping and sequence analysis was used to compare TCR clonotype distributions.

RESULTS

TCR-specific mRNA was detected in all synovial tissue biopsies at the first sampling, but in only 8/12 biopsies 16 weeks later (4/7 CSA group, 4/5 placebo group). Overrepresented TCR BV genes were found in biopsies of 10/12 patients at the first time point, and in 7/12 patients after 16 weeks (3/7 CSA, 4/5 placebo). CDR3 sequence analysis revealed dynamic repertoire changes with only a few persisting clonotypes in the synovial tissue of placebo controls. Persisting T cell clonotypes were more frequently found in the synovial tissue of CSA treated patients compared to the placebo group.

CONCLUSION

These data suggest a dynamic process of T cell recruitment in the joints of RA patients. This process, possibly due to activation and subsequent infiltration of new T cell clones, apparently is influenced by CSA treatment. Synovial tissue T cells were no longer detected after 16 weeks' CSA treatment in 3 patients. In the other CSA treated patients, new T cell clones infiltrated, while other clones were persistently represented in the joints. These data may have important consequences for the design of T cell targeted therapies for RA.

摘要

目的

研究早期类风湿关节炎(RA)患者滑膜组织中T细胞受体(TCR)库在16周内的变化;并研究环孢素A(CSA)对这些患者亚组中TCR库的影响。

方法

在两个时间点从12例早期RA患者获取滑膜组织活检样本和配对的血液样本。7例患者接受CSA(新山地明 - 环孢素,3mg/kg/天)治疗,5例患者接受安慰剂治疗,为期16周。通过半定量PCR - ELISA分析TCR V基因库。采用CDR3谱型分析和序列分析比较TCR克隆型分布。

结果

首次采样时,所有滑膜组织活检样本均检测到TCR特异性mRNA,但16周后仅在8/12例活检样本中检测到(CSA组4/7例,安慰剂组4/5例)。在首次采样时,10/12例患者的活检样本中发现TCR BV基因过度表达,16周后在7/12例患者中发现(CSA组3/7例,安慰剂组4/5例)。CDR3序列分析显示TCR库动态变化,安慰剂对照组滑膜组织中仅有少数克隆型持续存在。与安慰剂组相比,CSA治疗患者的滑膜组织中更频繁地发现持续存在的T细胞克隆型。

结论

这些数据表明RA患者关节中T细胞募集是一个动态过程。这个过程可能是由于新的T细胞克隆的激活和随后的浸润,显然受CSA治疗的影响。3例患者接受CSA治疗16周后滑膜组织中未再检测到T细胞。在其他接受CSA治疗的患者中,新的T细胞克隆浸润,而其他克隆型持续存在于关节中。这些数据可能对RA的T细胞靶向治疗设计具有重要意义。

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